Your search keyword '"Statland, Jeffrey M."' showing total 45 results

1. Longitudinal course of neurofilament light chain levels in amyotrophic lateral sclerosis—insights from a completed randomized controlled trial with rasagiline.

Author

Witzel, Simon, Statland, Jeffrey M., Steinacker, Petra, Otto, Markus, Dorst, Johannes, Schuster, Joachim, Barohn, Richard J., and Ludolph, Albert C.

Subjects

*AMYOTROPHIC lateral sclerosis, *RANDOMIZED controlled trials, *CYTOPLASMIC filaments, *CLUSTER randomized controlled trials, *DISEASE progression, *DISEASE duration

Abstract

Background and purpose: Rasagiline might be disease modifying in patients with amyotrophic lateral sclerosis (ALS). The aim was to evaluate the effect of rasagiline 2 mg/day on neurofilament light chain (NfL), a prognostic biomarker in ALS. Methods: In 65 patients with ALS randomized in a 3:1 ratio to rasagiline 2 mg/day (n = 48) or placebo (n = 17) in a completed randomized controlled multicentre trial, NfL levels in plasma were measured at baseline, month 6 and month 12. Longitudinal changes in NfL levels were evaluated regarding treatment and clinical parameters. Results: Baseline NfL levels did not differ between the study arms and correlated with disease progression rates both pre‐baseline (r = 0.64, p < 0.001) and during the study (r = 0.61, p < 0.001). NfL measured at months 6 and 12 did not change significantly from baseline in both arms, with a median individual NfL change of +1.4 pg/mL (interquartile range [IQR] −5.6, 14.2) across all follow‐up time points. However, a significant difference in NfL change at month 12 was observed between patients with high and low NfL baseline levels treated with rasagiline (high [n = 13], −6.9 pg/mL, IQR −20.4, 6.0; low [n = 18], +5.9 pg/mL, IQR −1.4, 19.7; p = 0.025). Additionally, generally higher longitudinal NfL variability was observed in patients with high baseline levels, whereas disease progression rates and disease duration at baseline had no impact on the longitudinal NfL course. Conclusion: Post hoc NfL measurements in completed clinical trials are helpful in interpreting NfL data from ongoing and future interventional trials and could provide hypothesis‐generating complementary insights. Further studies are warranted to ultimately differentiate NfL response to treatment from other factors. [ABSTRACT FROM AUTHOR]

Published

2024

2. Randomized phase 2 study of ACE‐083, a muscle‐promoting agent, in facioscapulohumeral muscular dystrophy.

Author

Statland, Jeffrey M., Campbell, Craig, Desai, Urvi, Karam, Chafic, Díaz‐Manera, Jordi, Guptill, Jeffrey T., Korngut, Lawrence, Genge, Angela, Tawil, Rabi N., Elman, Lauren, Joyce, Nanette C., Wagner, Kathryn R., Manousakis, Georgios, Amato, Anthony A., Butterfield, Russell J., Shieh, Perry B., Wicklund, Matthew, Gamez, Josep, Bodkin, Cynthia, and Pestronk, Alan

Abstract

Introduction/Aims: Facioscapulohumeral muscular dystrophy (FSHD) is a slowly progressive muscular dystrophy without approved therapies. In this study we evaluated whether locally acting ACE‐083 could safely increase muscle volume and improve functional outcomes in adults with FSHD. Methods: Participants were at least 18 years old and had FSHD1/FSHD2. Part 1 was open label, ascending dose, assessing safety and tolerability (primary objective). Part 2 was randomized, double‐blind for 6 months, evaluating ACE‐083240 mg/muscle vs placebo injected bilaterally every 3 weeks in the biceps brachii (BB) or tibialis anterior (TA) muscles, followed by 6 months of open label. Magnetic resonance imaging measures included total muscle volume (TMV; primary objective), fat fraction (FF), and contractile muscle volume (CMV). Functional measures included 6‐minute walk test, 10‐meter walk/run, and 4‐stair climb (TA group), and performance of upper limb midlevel/elbow score (BB group). Strength, patient‐reported outcomes (PROs), and safety were also evaluated. Results: Parts 1 and 2 enrolled 37 and 58 participants, respectively. Among 55 participants evaluable in Part 2, the least‐squares mean (90% confidence interval, analysis of covariance) treatment difference for TMV was 16.4% (9.8%‐23.0%) in the BB group (P <.0001) and 9.5% (3.2%‐15.9%) in the TA group (P =.01). CMV increased significantly in the BB and TA groups and FF decreased in the TA group. There were no consistent improvements in functional or PRO measures in either group. The most common adverse events were mild or moderate injection‐site reactions. Discussion: Significant increases in TMV with ACE‐083 vs placebo did not result in consistent functional or PRO improvements with up to 12 months of treatment. [ABSTRACT FROM AUTHOR]

Published

2022

3. A pilot study of the responsiveness of wireless motion analysis in facioscapulohumeral muscular dystrophy.

Author

Statland, Jeffrey M., Karanevich, Alex, Bruetsch, Adam, and Huisinga, Jessie

Subjects

*COMPARATIVE studies, *RANGE of motion of joints, *LONGITUDINAL method, *RESEARCH methodology, *MEDICAL cooperation, *MUSCULAR dystrophy, *RESEARCH, *RESEARCH funding, *WIRELESS communications, *PILOT projects, *EVALUATION research, *DISEASE progression

Abstract

Introduction: We determined whether instrumenting timed functional tasks with wireless inertial motion sensors were responsive to facioscapulohumeral muscular dystrophy (FSHD) progression and movement pattern changes.Methods: Ten individuals who were clinically affected with genetically confirmed FSHD, mean age 54 years (range 42-65), performed an instrumented timed up and go (iTUG) trial at each visit, wearing six wireless inertial sensors. We determined the estimated average monthly slope of progression and 12-month change for temporal and spatial motion variables using a linear mixed effects model.Results: For an average of 20.6 months (range 6.1-34.5), the iTUG duration stayed constant, whereas stride length, stride velocity, and trunk sagittal range of motion changed, indicating poorer performance. Arm swing changed in a compensatory direction toward the normative mean.Discussion: This study provides preliminary evidence that iTUG motion variables could be sensitive to progression in FSHD, but this requires validation in a larger study. [ABSTRACT FROM AUTHOR]

Published

2019

4. Rasagiline for amyotrophic lateral sclerosis: A randomized, controlled trial.

Author

Statland, Jeffrey M., Moore, Dan, Wang, Yunxia, Walsh, Maureen, Mozaffar, Tahseen, Elman, Lauren, Nations, Sharon P., Mitsumoto, Hiroshi, Fernandes, J. Americo, Saperstein, David, Hayat, Ghazala, Herbelin, Laura, Karam, Chafic, Katz, Jonathan, Wilkins, Heather M., Agbas, Abdulbaki, Swerdlow, Russell H., Santella, Regina M., Dimachkie, Mazen M., and Barohn, Richard J.

Subjects

*AMYOTROPHIC lateral sclerosis, *COMPARATIVE studies, *HYDROCARBONS, *RESEARCH methodology, *MEDICAL cooperation, *HEALTH outcome assessment, *QUALITY of life, *RESEARCH, *RESEARCH funding, *DNA-binding proteins, *EVALUATION research, *RANDOMIZED controlled trials, *TREATMENT effectiveness, *NEUROPROTECTIVE agents, *BLIND experiment, *RETROSPECTIVE studies, *SEVERITY of illness index

Abstract

Introduction: Rasagiline is a monoamine oxidase B (MAO-B) inhibitor with possible neuroprotective effects in patients with amyotrophic lateral sclerosis (ALS).Methods: We performed a randomized, double-blind, placebo-controlled trial of 80 ALS participants with enrichment of the placebo group with historical controls (n = 177) at 10 centers in the United States. Participants were randomized in a 3:1 ratio to 2 mg/day rasagiline or placebo. The primary outcome was average slope of decline on the ALS Functional Rating Scale-Revised (ALSFRS-R). Secondary measures included slow vital capacity, survival, mitochondrial and molecular biomarkers, and adverse-event reporting.Results: There was no difference in the average 12-month ALSFRS-R slope between rasagiline and the mixed placebo and historical control cohorts. Rasagiline did not show signs of drug-target engagement in urine and blood biomarkers. Rasagiline was well tolerated with no serious adverse events.Discussion: Rasagiline did not alter disease progression compared with controls over 12 months of treatment. Muscle Nerve 59:201-207, 2019. [ABSTRACT FROM AUTHOR]

Published

2019

5. Review of the Diagnosis and Treatment of Periodic Paralysis.

Author

Statland, Jeffrey M., Fontaine, Bertrand, Hanna, Michael G., Johnson, Nicholas E., Kissel, John T., Sansone, Valeria A., Shieh, Perry B., Tawil, Rabi N., Trivedi, Jaya, Cannon, Stephen C., and Griggs, Robert C.

Subjects

*ACETAZOLAMIDE, *BEHAVIOR therapy, *DIURETICS, *INBORN errors of metabolism, *METALS in the body, *MYOCARDIAL depressants, *POTASSIUM, *RESEARCH funding, *HEALTH self-care, *SELF-evaluation, *ANDERSEN syndrome, *HYDROCHLOROTHIAZIDE, *CARBONIC anhydrase inhibitors, *POTASSIUM-sparing diuretics, INBORN errors of metabolism diagnosis

Abstract

Periodic paralyses (PPs) are rare neuromuscular disorders caused by mutations in skeletal muscle sodium, calcium, and potassium channel genes. PPs include hypokalemic paralysis, hyperkalemic paralysis, and Andersen-Tawil syndrome. Common features of PP include autosomal dominant inheritance, onset typically in the first or second decades, episodic attacks of flaccid weakness, which are often triggered by diet or rest after exercise. Diagnosis is based on the characteristic clinic presentation then confirmed by genetic testing. In the absence of an identified genetic mutation, documented low or high potassium levels during attacks or a decrement on long exercise testing support diagnosis. The treatment approach should include both management of acute attacks and prevention of attacks. Treatments include behavioral interventions directed at avoidance of triggers, modification of potassium levels, diuretics, and carbonic anhydrase inhibitors. Muscle Nerve 57: 522-530, 2018. [ABSTRACT FROM AUTHOR]

Published

2018

6. Electrical impedance myography in facioscapulohumeral muscular dystrophy.

Author

Statland, Jeffrey M., Heatwole, Chad, Eichinger, Katy, Dilek, Nuran, Martens, William B., and Tawil, Rabi

Subjects

*MUSCULAR dystrophy diagnosis, *DIAGNOSIS, *BIOELECTRIC impedance, *LONGITUDINAL method, *MUSCLES, *MUSCULAR dystrophy, *RESEARCH funding, *CROSS-sectional method, *SKELETAL muscle

Abstract

Introduction: In this study we determined the reliability and validity of electrical impedance myography (EIM) in facioscapulohumeral muscular dystrophy (FSHD).Methods: We performed a prospective study of EIM on 16 bilateral limb and trunk muscles in 35 genetically defined and clinically affected FSHD patients (reliability testing on 18 patients). Summary scores based on body region were derived. Reactance and phase (50 and 100 kHz) were compared with measures of strength, FSHD disease severity, and functional outcomes.Results: Participants were mostly men, mean age 53.0 years, and included a full range of severity. Limb and trunk muscles showed good to excellent reliability [intraclass correlation coefficients (ICC) 0.72-0.99]. Summary scores for the arm, leg, and trunk showed excellent reliability (ICC 0.89-0.98). Reactance was the most sensitive EIM parameter to a broad range of FSHD disease metrics.Conclusions: EIM is a reliable measure of muscle composition in FSHD that offers the possibility to serially evaluate affected muscles. Muscle Nerve 54: 696-701, 2016. [ABSTRACT FROM AUTHOR]

Published

2016

7. Muscle pathology grade for facioscapulohumeral muscular dystrophy biopsies.

Author

Statland, Jeffrey M., Shah, Bharati, Henderson, Don, Van Der Maarel, Silvere, Tapscott, Stephen J., and Tawil, Rabi

Subjects

*RANGE of motion of joints, *LONGITUDINAL method, *MUSCULAR dystrophy, *NEEDLE biopsy, *RESEARCH funding, *CD4 antigen, *CROSS-sectional method, *SEVERITY of illness index, *SKELETAL muscle

Abstract

Introduction: As we move toward planning for clinical trials in facioscapulohumeral muscular dystrophy (FSHD), a better understanding of the clinical relationship with morphological changes in FSHD muscle biopsies will be important for stratifying patients and understanding post-therapeutic changes in muscle.Methods: We performed a prospective cross-sectional study of quadriceps muscle biopsies in 74 genetically confirmed FSHD participants (64 with FSHD type 1 and 10 with FSHD type 2). We compared a 12-point muscle pathology grade to genetic mutation, disease severity score, and quantitative myometry.Results: Pathology grade had moderate correlations with genetic mutation (rho = -0.45, P < 0.001), clinical severity score (rho = 0.53, P < 0.001), disease duration (rho = 0.31, P = 0.03), and quantitative myometry (rho = -0.47, P < 0.001). We found no difference in the frequency of inflammation between FSHD types 1 and 2.Conclusions: The pathology grade of quadriceps muscle may be a useful marker of disease activity in FSHD, and it may have a role in stratification for future clinical trials. [ABSTRACT FROM AUTHOR]

Published

2015

8. Risk of functional impairment in Facioscapulohumeral muscular dystrophy.

Author

Statland, Jeffrey M. and Tawil, Rabi

Abstract

ABSTRACT Introduction: Facioscapulohumeral muscular dystrophy (FSHD) is one of the most prevalent muscular dystrophies. Nevertheless, little is known about the risk of developing functional impairment. Here we determine the 6-year risk of functional impairment in FSHD. Methods: A retrospective cohort of 313 genetically confirmed, clinically affected FSHD participants in a United States registry between January 2002 and June 2011. Our main outcome was wheelchair (WC) use. Results: The 6-year risk of WC use was 24.0% (95% confidence interval 18.6-29.3). The distribution of WC risk was bimodal, with a peak in the second decade associated with large D4Z4 contractions, followed by an age-related increase in risk. Other functional categories showed moderate risk. Prevalence of hearing aid use and difficulty pronouncing words was increased in large D4Z4 contractions. Conclusions: The 6-year risk of functional impairment in FSHD is moderate, and early WC use is associated with large D4Z4 contractions. Muscle Nerve 49:520-527, 2014 [ABSTRACT FROM AUTHOR]

Published

2014

9. The diagnosis and treatment of myotonic disorders.

Author

Heatwole, Chad R., Statland, Jeffrey M., and Logigian, Eric L.

Abstract

Myotonia is a defining clinical symptom and sign common to a relatively small group of muscle diseases, including the myotonic dystrophies and the nondystrophic myotonic disorders. Myotonia can be observed on clinical examination, as can its electrical correlate, myotonic discharges, on electrodiagnostic testing. Research interest in the myotonic disorders continues to expand rapidly, which justifies a review of the scientific bases, clinical manifestations, and numerous therapeutic approaches associated with these disorders. We review the pathomechanisms of myotonia, the clinical features of the dystrophic and nondystrophic myotonic disorders, and the diagnostic approach and treatment options for patients with symptomatic myotonia. Muscle Nerve 47: 632-648, 2013 [ABSTRACT FROM AUTHOR]

Published

2013

10. Reevaluating measures of disease progression in facioscapulohumeral muscular dystrophy

Author

Statland, Jeffrey M., McDermott, Michael P., Heatwole, Chad, Martens, William B., Pandya, Shree, van der Kooi, E.L., Kissel, John T., Wagner, Kathryn R., and Tawil, Rabi

Subjects

*DISEASE progression, *FACIOSCAPULOHUMERAL muscular dystrophy, *PATHOLOGICAL physiology, *CLINICAL trials, *COMPARATIVE studies, *TARGETED drug delivery, *DIAGNOSIS

Abstract

Abstract: Recent advances in the understanding of the molecular pathophysiology of facioscapulohumeral muscular dystrophy (FSHD) have identified potential therapeutic targets. Consequently, an accurate understanding of disease progression in FSHD is crucial for the design of future clinical trials. Data from 228 subjects in 3 clinical trials and 1 natural history study were compared to examine disease progression in FSHD. All studies utilized the same techniques for manual muscle testing and maximum voluntary isometric contraction testing. Both techniques yield a total strength score that can be followed over time as an indicator of disease progression. Whereas natural history data showed a decrease in strength over 1year, there was an apparent increase in strength at 6months in 2 of the 3 clinical trials in both the placebo and treatment groups, that persisted for up to 1year for maximum voluntary isometric contraction testing. Variability estimates from the clinical trial data were consistent with those seen in the natural history data. Patients in clinical trials in FSHD may have better outcomes than those in natural history studies, regardless of treatment assignment, emphasizing the importance of placebo groups and the need for caution when interpreting the strength results of controlled and uncontrolled trials. [Copyright &y& Elsevier]

Published

2013

11. Mexiletine for Symptoms and Signs of Myotonia in Nondystrophic Myotonia: A Randomized Controlled Trial.

Author

Statland, Jeffrey M., Bundy, Brian N., Yunxia Wang, Raja Rayan, Dipa, Trivedi, Jaya R., Sansone, Valeria A., Salajegheh, Mohammad K., Venance, Shannon L., Ciafaloni, Emma, Matthews, Emma, Meola, Giovanni, Herbelin, Laura, Griggs, Robert C., Barohn, Richard J., and Hanna, Michael G.

Subjects

*MEXILETINE, *CLINICAL trials, *PLACEBOS, *MYOTONIA, *BLIND experiment, *INTERACTIVE voice response (Telecommunication), *PATIENTS, *ETHNICITY, *DIAGNOSIS

Abstract

The article informs about a study based on clinical trial related with assessment of the effects of mexiletine for symptoms and signs of myotonia in Nondystrophic myotonias (NDMs) patients. It mentions that randomized, doubleblind and placebo-controlled approach was used in the study. It includes that participants were randomly given mexiletine or placebo capsules and adds that baseline characteristics includes sex, age, and self-reported ethnicity of the patients. It also includes that patient-reported severity score of stiffness is recorded on an interactive voice response (IVR) diary. According to the study, the use of mexiletine compared with placebo resulted in improved patient-reported stiffness.

Published

2012

12. A quantitative measure of handgrip myotonia in non-dystrophic myotonia.

Author

Statland, Jeffrey M., Bundy, Brian N., Wang, Yunxia, Trivedi, Jaya R., Raja Rayan, Dipa, Herbelin, Laura, Donlan, Merideth, McLin, Rhonda, Eichinger, Katy J., Findlater, Karen, Dewar, Liz, Pandya, Shree, Martens, William B., Venance, Shannon L., Matthews, Emma, Amato, Anthony A., Hanna, Michael G., Griggs, Robert C., and Barohn, Richard J.

Abstract

Introduction: Non-dystrophic myotonia (NDM) is characterized by myotonia without muscle wasting. A standardized quantitative myotonia assessment (QMA) is important for clinical trials. Methods: Myotonia was assessed in 91 individuals enrolled in a natural history study using a commercially available computerized handgrip myometer and automated software. Average peak force and 90% to 5% relaxation times were compared with historical normal controls studied with identical methods. Results: Thirty subjects had chloride channel mutations, 31 had sodium channel mutations, 6 had DM2 mutations, and 24 had no identified mutation. Chloride channel mutations were associated with prolonged first handgrip relaxation times and warm-up on subsequent handgrips. Sodium channel mutations were associated with prolonged first handgrip relaxation times and paradoxical myotonia or warm-up, depending on underlying mutations. DM2 subjects had normal relaxation times but decreased peak force. Sample size estimates are provided for clinical trial planning. Conclusion: QMA is an automated, non-invasive technique for evaluating myotonia in NDM. Muscle Nerve 46: 482-489, 2012 [ABSTRACT FROM AUTHOR]

Published

2012

13. An interactive voice response diary for patients with non-dystrophic myotonia.

Author

Statland, Jeffrey M., Wang, Yunxia, Richesson, Rachel, Bundy, Brian, Herbelin, Laura, Gomes, Joe, Trivedi, Jaya, Venance, Shannon, Amato, Anthony, Hanna, Michael, Griggs, Robert, and Barohn, Richard J.

Abstract

Introduction: Non-dystrophic myotonia (NDM) is caused by mutations in muscle chloride and sodium channels. Currently, there is no standardized instrument for documenting symptom frequency and severity in NDM. Methods: Subjects used an automated, interactive, telephone-based voice response diary (IVR) to record frequency and severity of stiffness, weakness, pain, and tiredness once a week for 8 weeks, after their baseline visits. Results: We describe the IVR and report data on 76 subjects for a total of 385 person-weeks. Overall there were 5.1 calls per subject. Forty-eight subjects called in 5 or more times, and 14 called in 8 times. Stiffness was both the most frequent and severe symptom. Warm-up and handgrip myotonia were associated with higher severity scores for stiffness. Conclusions: IVR is a convenient technology to allow patient reporting of repeated and real-time symptom frequency and severity, and it is presently being used in a trial of mexiletine in NDM. Muscle Nerve 44: 30-35, 2011 [ABSTRACT FROM AUTHOR]

Published

2011

14. Primary lateral sclerosis.

Author

Singer, Mike A., Statland, Jeffrey M., Wolfe, Gil I., and Barohn, Richard J.

Abstract

The spectrum of motor neuron diseases ranges from disorders that clinically are limited to lower motor neurons to those that exclusively affect upper motor neurons. Primary lateral sclerosis (PLS) is the designation for the syndrome of progressive upper motor neuron dysfunction when no other etiology is identified. Distinction between PLS and the more common amyotrophic lateral sclerosis (ALS) relies primarily on recognition of their symptoms and signs, as well as on ancillary, although non-specific, laboratory data. In this review, we survey the history of PLS from the initial descriptions to the present. We discuss the role of laboratory, electrodiagnostic, and imaging studies in excluding other diagnoses; the findings from major case series of PLS patients; and proposed diagnostic criteria. Consistent differences are evident in patients classified as PLS compared to those with ALS, indicating that, despite its limitations, this clinical designation retains important utility. Muscle Nerve, 2007 [ABSTRACT FROM AUTHOR]

Published

2007

15. Cell type-specific dependence of muscarinic signalling in mouse hippocampal stratum oriens interneurones.

Author

Lawrence, J. Josh, Statland, Jeffrey M., Grinspan, Zachary M., and McBain, Chris J.

Subjects

*HIPPOCAMPUS (Brain), *PARASYMPATHOMIMETIC agents, *INTERNEURONS, *AXONS, *CEREBRAL cortex, *LIMBIC system

Abstract

Cholinergic signalling is critically involved in learning and memory processes in the hippocampus, but the postsynaptic impact of cholinergic modulation on morphologically defined subtypes of hippocampal interneurones remains unclear. We investigated the influence of muscarinic receptor (mAChR) activation on stratum oriens interneurones using whole-cell patch clamp recordings from hippocampal slices in vitro. Upon somatic depolarization, mAChR activation consistently enhanced firing frequency and produced large, sustained afterdepolarizations (ADPs) of stratum oriens–lacunosum moleculare (O-LM) interneurones. In contrast, stratum oriens cell types with axon arborization patterns different from O-LM cells not only lacked large muscarinic ADPs but also appeared to exhibit distinct responses to mAChR activation. The ADP in O-LM cells, mediated by M1/M3 receptors, was associated with inhibition of an M current, inhibition of a slow calcium-activated potassium current, and activation of a calcium-dependent non-selective cationic current ( ICAT). An examination of ionic conductances generated by firing revealed that calcium entry through ICAT controls the emergence of the mAChR-mediated ADP. Our results indicate that cholinergic specializations are present within anatomically distinct subpopulations of hippocampal interneurones, suggesting that there may be organizing principles to cholinergic control of GABA release in the hippocampus. [ABSTRACT FROM AUTHOR]

Published

2006

16. Self-reported reduced sleep quality and excessive daytime sleepiness in facioscapulohumeral muscular dystrophy.

Author

Hoffmann, Heloise M., Malo‐Juvera, Victor, Statland, Jeffrey M., and Malo-Juvera, Victor

Abstract

Introduction/aims: Facioscapulohumeral muscular dystrophy (FSHD) causes weakness and secondary associations, such as respiratory complications and pain, that can be linked to abnormal sleep patterns. Limited studies have focused on sleep in FSHD. The purpose of this study was to identify the prevalence of, and clinical features associated with, self-reported lowered sleep quality (SQ) and excessive daytime sleepiness (DS) in a large group of participants with FSHD.Methods: We conducted a prospective survey of individuals with self-reported FSHD enrolled in the FSHD Society Registry. The survey consisted of demographic and clinical characteristics, the Pittsburgh Sleep Quality Index (PSQI), and the Epworth Sleepiness Scale. Descriptive statistics were evaluated, and associations between clinical characteristics and SQ and DS were explored using one-way analysis of variance tests. Small effect size was identified as 0.01 ≥ η2  > 0.06, medium was 0.06 ≥ η2  > 0.14, and large was 0.14 ≥ η2 .Results: Six hundred ninety individuals responded to the survey, equally distributed between men and women, and spanning the age range from under 12 to 74 years of age or older. Sixty-six percent of the respondents showed reduced SQ (PSQI > 5) (n = 392; 95% confidence interval [CI], 62.4-70.0), and 15% showed excessive DS (>10) (n = 89; 95% CI, 12.2-17.9). There was a significant association between SQ and DS. Nocturnal pain had a large significant effect on lowering SQ (P < .001, η2  = 0.192). Factors including age and gender had minor effects on SQ.Discussion: Physicians should monitor sleep quality of patients with FSHD as a routine part of care, with special attention to potentially modifiable factors. Future research should address the physiological effects of pain in sleep. [ABSTRACT FROM AUTHOR]

Published

2022

17. Challenges and opportunities for Multi-National Investigator-Initiated clinical trials for ALS: European and United States collaborations.

Author

Lingor, Paul, Koch, Jan C., Statland, Jeffrey M., Hussain, Sumaira, Hennecke, Christiane, Wuu, Joanne, Langbein, Thomas, Ahmed, Raees, Günther, René, Ilse, Benjamin, Kassubek, Jan, Kollewe, Katja, Kuttler, Josua, Leha, Andreas, Lengenfeld, Teresa, Meyer, Thomas, Neuwirth, Christoph, Tostmann, Ralf, and Benatar, Michael

Subjects

*CLINICAL trials, *AMYOTROPHIC lateral sclerosis

Abstract

An inherent challenge to clinical trials that aim to test the efficacy of experimental therapeutics for patients with amyotrophic lateral sclerosis (ALS) is the relative rarity of the disease. A promising solution to this problem is a multi-center approach that ideally includes sites distributed across a broad geographic area. In support of such an approach, the European E-RARE program and the United States National Institutes of Health (NIH) partnered to support the investigator-initiated ROCK-ALS trial (Eudra-CT-Nr.: 2017-003676-31, NCT03792490) as a multi-national collaboration between centers in Europe and North America that is led by European investigators. During the set-up of this international trial, however, a number of unanticipated legal, administrative, and financial complexities emerged that required significant adaptation of the proposed trial scheme. Here, we report our experience navigating these obstacles and describe the potential solutions that we explored. Our experience may inform future efforts to implement multi-national investigator-initiated trials that involve both European and United States centers. [ABSTRACT FROM AUTHOR]

Published

2021

18. Safety and efficacy of losmapimod in facioscapulohumeral muscular dystrophy (ReDUX4): a randomised, double-blind, placebo-controlled phase 2b trial.

Author

Tawil, Rabi, Wagner, Kathryn R, Hamel, Johanna I, Leung, Doris G, Statland, Jeffrey M, Wang, Leo H, Genge, Angela, Sacconi, Sabrina, Lochmüller, Hanns, Reyes-Leiva, David, Diaz-Manera, Jordi, Alonso-Perez, Jorge, Muelas, Nuria, Vilchez, Juan J, Pestronk, Alan, Gibson, Summer, Goyal, Namita A, Hayward, Lawrence J, Johnson, Nicholas, and LoRusso, Samantha

Subjects

*FACIOSCAPULOHUMERAL muscular dystrophy, *SURGICAL site infections, *TERMINATION of treatment, *ALCOHOL poisoning, *SHOULDER girdle, *SMALL molecules

Abstract

Facioscapulohumeral muscular dystrophy is a hereditary progressive myopathy caused by aberrant expression of the transcription factor DUX4 in skeletal muscle. No approved disease-modifying treatments are available for this disorder. We aimed to assess the safety and efficacy of losmapimod (a small molecule that inhibits p38α MAPK, a regulator of DUX4 expression, and p38β MAPK) for the treatment of facioscapulohumeral muscular dystrophy. We did a randomised, double-blind, placebo-controlled phase 2b trial at 17 neurology centres in Canada, France, Spain, and the USA. We included adults aged 18–65 years with type 1 facioscapulohumeral muscular dystrophy (ie, with loss of repression of DUX4 expression, as ascertained by genotyping), a Ricci clinical severity score of 2–4, and at least one skeletal muscle judged using MRI to be suitable for biopsy. Participants were randomly allocated (1:1) to either oral losmapimod (15 mg twice a day) or matching placebo for 48 weeks, via an interactive response technology system. The investigator, study staff, participants, sponsor, primary outcome assessors, and study monitor were masked to the treatment allocation until study closure. The primary endpoint was change from baseline to either week 16 or 36 in DUX4-driven gene expression in skeletal muscle biopsy samples, as measured by quantitative RT-PCR. The primary efficacy analysis was done in all participants who were randomly assigned and who had available data for assessment, according to the modified intention-to-treat principle. Safety and tolerability were assessed as secondary endpoints. This study is registered at ClinicalTrials.gov , number NCT04003974. The phase 2b trial is complete; an open-label extension is ongoing. Between Aug 27, 2019, and Feb 27, 2020, 80 people were enrolled. 40 were randomly allocated to losmapimod and 40 to placebo. 54 (68%) participants were male and 26 (33%) were female, 70 (88%) were White, and mean age was 45·7 (SD 12·5) years. Least squares mean changes from baseline in DUX4 - driven gene expression did not differ significantly between the losmapimod (0·83 [SE 0·61]) and placebo (0·40 [0·65]) groups (difference 0·43 [SE 0·56; 95% CI –1·04 to 1·89]; p=0·56). Losmapimod was well tolerated. 29 treatment-emergent adverse events (nine drug-related) were reported in the losmapimod group compared with 23 (two drug-related) in the placebo group. Two participants in the losmapimod group had serious adverse events that were deemed unrelated to losmapimod by the investigators (alcohol poisoning and suicide attempt; postoperative wound infection) compared with none in the placebo group. No treatment discontinuations due to adverse events occurred and no participants died during the study. Although losmapimod did not significantly change DUX4-driven gene expression, it was associated with potential improvements in prespecified structural outcomes (muscle fat infiltration), functional outcomes (reachable workspace, a measure of shoulder girdle function), and patient-reported global impression of change compared with placebo. These findings have informed the design and choice of efficacy endpoints for a phase 3 study of losmapimod in adults with facioscapulohumeral muscular dystrophy. Fulcrum Therapeutics. [ABSTRACT FROM AUTHOR]

Published

2024

19. Using an onset-anchored Bayesian hierarchical model to improve predictions for amyotrophic lateral sclerosis disease progression.

Author

Karanevich, Alex G., Statland, Jeffrey M., Gajewski, Byron J., and He, Jianghua

Subjects

*AMYOTROPHIC lateral sclerosis, *DISEASE progression, *HIERARCHICAL Bayes model, *BAYESIAN analysis, *PREDICTION models

Abstract

Background: Amyotrophic Lateral Sclerosis (ALS), also known as Lou Gehrig's disease, is a rare disease with extreme between-subject variability, especially with respect to rate of disease progression. This makes modelling a subject's disease progression, which is measured by the ALS Functional Rating Scale (ALSFRS), very difficult. Consider the problem of predicting a subject's ALSFRS score at 9 or 12 months after a given time-point.Methods: We obtained ALS subject data from the Pooled Resource Open-Access ALS Clinical Trials Database, a collection of data from various ALS clinical trials. Due to the typical linearity of the ALSFRS, we consider several Bayesian hierarchical linear models. These include a mixture model (to account for the two potential classes of "fast" and "slow" ALS progressors) as well as an onset-anchored model, in which an additional artificial data-point, using time of disease onset, is utilized to improve predictive performance.Results: The onset-anchored model had a drastically reduced posterior predictive mean-square-error distributions, when compared to the Bayesian hierarchical linear model or the mixture model under a cross-validation approach. No covariates, other than time of disease onset, consistently improved predictive performance in either the Bayesian hierarchical linear model or the onset-anchored model.Conclusions: Augmenting patient data with an additional artificial data-point, or onset anchor, can drastically improve predictive modelling in ALS by reducing the variability of estimated parameters at the cost of a slight increase in bias. This onset-anchored model is extremely useful if predictions are desired directly after a single baseline measure (such as at the first day of a clinical trial), a feat that would be very difficult without the onset-anchor. This approach could be useful in modelling other diseases that have bounded progression scales (e.g. Parkinson's disease, Huntington's disease, or inclusion-body myositis). It is our hope that this model can be used by clinicians and statisticians to improve the efficacy of clinical trials and aid in finding treatments for ALS. [ABSTRACT FROM AUTHOR]

Published

2018

20. Phase 2 trial in acetylcholine receptor antibody‐positive myasthenia gravis of transition from intravenous to subcutaneous immunoglobulin: The MGSCIg study.

Author

Pasnoor, Mamatha, Bril, Vera, Levine, Todd, Trivedi, Jaya, Silvestri, Nicholas J., Phadnis, Milind, Katzberg, Hans D., Saperstein, David S., Wolfe, Gil I., Herbelin, Laura, Higgs, Kiley, Heim, Andrew J., Statland, Jeffrey M., Barohn, Richard J., and Dimachkie, Mazen M.

Subjects

*MYASTHENIA gravis, *CHOLINERGIC receptors, *PATIENT satisfaction, *CLINICAL deterioration, *CLINICAL medicine, *INTRAVENOUS immunoglobulins

Abstract

Background and purpose: Data on maintenance therapy with subcutaneous immunoglobulin (SCIg) in myasthenia gravis (MG) are limited. We report on transitioning acetylcholine receptor (AChR) antibody‐positive (Ab+) MG patients on stable intravenous immunoglobulin (IVIg) regimens as part of routine clinical care to SCIg 1:1.2. Methods: This multicenter North American open‐label prospective investigator‐initiated study had two components: the IVIg Stabilization Period (ISP) enrolling patients already on IVIg as part of routine clinical care (Weeks −10 to −1), followed by transition of stable MG subjects to SCIg in the Experimental Treatment Period (ETP; Weeks 0 to 12). We hypothesized that >65% of patients entering the ETP would have a stable Quantitative Myasthenia Gravis (QMG) score from Week 0 to Week 12. Secondary outcome measures included other efficacy measures, safety, tolerability, IgG levels, and treatment satisfaction. Results: We recruited 23 patients in the ISP, and 22 entered the ETP. A total of 12 subjects (54.5%) were female, and 18 (81.8%) were White, with mean age 51.4 ± 17 years. We obtained Week 12 ETP QMG data on 19 of 22; one subject withdrew from ETP owing to clinical deterioration, and two subjects withdrew due to dislike of needles. On primary analysis, 19 of 22 participants (86.4%, 95% confidence interval = 0.72–1.00) were treatment successes using last observation carried forward (p = 0.018). Secondary efficacy measures supported MG stability. SCIg was safe and well tolerated, and IgG levels were stable. Treatment satisfaction was comparable between ISP and ETP. Conclusions: MG patients on IVIg as part of their routine clinical care remained stable on monthly IVIg dosage, and most maintained similar disease stability on SCIg. [ABSTRACT FROM AUTHOR]

Published

2023

21. Facioscapulohumeral muscular dystrophy: the road to targeted therapies.

Author

Tihaya, Mara S., Mul, Karlien, Balog, Judit, de Greef, Jessica C., Tapscott, Stephen J., Tawil, Rabi, Statland, Jeffrey M., and van der Maarel, Silvère M.

Subjects

*FACIOSCAPULOHUMERAL muscular dystrophy, *MYOSITIS, *MUSCLE weakness, *GENE expression, *SHOULDER girdle, *FACIAL muscles

Abstract

Advances in the molecular understanding of facioscapulohumeral muscular dystrophy (FSHD) have revealed that FSHD results from epigenetic de-repression of the DUX4 gene in skeletal muscle, which encodes a transcription factor that is active in early embryonic development but is normally silenced in almost all somatic tissues. These advances also led to the identification of targets for disease-altering therapies for FSHD, as well as an improved understanding of the molecular mechanism of the disease and factors that influence its progression. Together, these developments led the FSHD research community to shift its focus towards the development of disease-modifying treatments for FSHD. This Review presents advances in the molecular and clinical understanding of FSHD, discusses the potential targeted therapies that are currently being explored, some of which are already in clinical trials, and describes progress in the development of FSHD-specific outcome measures and assessment tools for use in future clinical trials. Facioscapulohumeral muscular dystrophy is caused by aberrant expression of the transcription factor DUX4. Tihaya, Mul and colleagues describe advances in the development of targeted treatments for facioscapulohumeral muscular dystrophy and discuss potential clinical trial outcome measures as well as molecular and imaging biomarkers. Key points: Facioscapulohumeral muscular dystrophy (FSHD), a disorder for which there currently is no cure, is characterized by muscle weakness, predominantly affecting muscles in the face, shoulder girdle and upper arms. FSHD is associated with epigenetic de-repression of the DUX4 gene, which leads to aberrant expression of the transcription factor DUX4 and cytotoxicity in skeletal muscle cells. Clinical disease progression occurs in a nonlinear and muscle-by-muscle fashion with phases of muscle inflammation preceding rapid fatty replacement of muscle tissue and muscle wasting. Consensus has been reached on the pathogenetic mechanism of FSHD, and the field is entering a new era of targeted therapy development. Disease-altering therapies currently in development range from proof-of-principle gene-editing technologies focusing on reducing DUX4 expression to clinical trials of DUX4-blocking agents. Clinical trials in FSHD require the development of meaningful patient outcome measures, identification of reliable biomarkers and accurate methods of measuring disease progression, such as MRI and ultrasonography. [ABSTRACT FROM AUTHOR]

Published

2023

22. Correction to: A double-blind, placebo-controlled, randomized trial of PXT3003 for the treatment of Charcot–Marie–Tooth type 1A.

Author

Attarian, Shahram, Young, Peter, Brannagan, Thomas H., Adams, David, Van Damme, Philip, Thomas, Florian P., Casanovas, Carlos, Kafaie, Jafar, Tard, Céline, Walter, Maggie C., Péréon, Yann, Walk, David, Stino, Amro, de Visser, Marianne, Verhamme, Camiel, Amato, Anthony, Carter, Gregory, Magy, Laurent, Statland, Jeffrey M., and Felice, Kevin

Subjects

*RARE diseases

Abstract

This document is a correction notice for an article titled "A double-blind, placebo-controlled, randomized trial of PXT3003 for the treatment of Charcot-Marie-Tooth type 1A" published in the Orphanet Journal of Rare Diseases. The correction adds an additional author, Jafar Kafaie, to the authors' group. The original article has been updated to reflect this change. The publisher, Springer Nature, remains neutral regarding jurisdictional claims and institutional affiliations. The article is authored by multiple individuals from various institutions. [Extracted from the article]

Published

2024

23. Non‐dystrophic myotonia: 2‐year clinical and patient reported outcomes.

Author

Fullam, Timothy R., Chandrashekhar, Swathy, Farmakidis, Constantine, Jawdat, Omar, Pasnoor, Mamatha, Dimachkie, Mazen M., and Statland, Jeffrey M.

Abstract

Introduction/Aims: Consistency of differences between non‐dystrophic myotonias over time measured by standardized clinical/patient‐reported outcomes is lacking. Evaluation of longitudinal data could establish clinically relevant endpoints for future research. Methods: Data from prospective observational study of 95 definite/clinically suspected non‐dystrophic myotonia participants (six sites in the United States, United Kingdom, and Canada) between March 2006 and March 2009 were analyzed. Outcomes included: standardized symptom interview/exam, Short Form‐36, Individualized Neuromuscular Quality of Life (INQoL), electrophysiological short/prolonged exercise tests, manual muscle testing, quantitative grip strength, modified get‐up‐and‐go test. Patterns were assigned as described by Fournier et al. Comparisons were restricted to confirmed sodium channelopathies (SCN4A, baseline, year 1, year 2: n = 34, 19, 13), chloride channelopathies (CLCN1, n = 32, 26, 18), and myotonic dystrophy type 2 (DM2, n = 9, 6, 2). Results: Muscle stiffness was the most frequent symptom over time (54.7%–64.7%). Eyelid myotonia and paradoxical handgrip/eyelid myotonia were more frequent in SCN4A. Grip strength and combined manual muscle testing remained stable. Modified get‐up‐and‐go showed less warm up in SCN4A but remained stable. Median post short exercise decrement was stable, except for SCN4A (baseline to year 2 decrement difference 16.6% [Q1, Q3: 9.5, 39.2]). Fournier patterns type 2 (CLCN1) and 1 (SCN4A) were most specific; 40.4% of participants had a change in pattern over time. INQoL showed higher impact for SCN4A and DM2 with scores stable over time. Discussion: Symptom frequency and clinical outcome assessments were stable with defined variability in myotonia measures supporting trial designs like cross over or combined n‐of‐1 as important for rare disorders. [ABSTRACT FROM AUTHOR]

Published

2022

24. Quantitative muscle analysis in facioscapulohumeral muscular dystrophy using whole‐body fat‐referenced MRI: Protocol development, multicenter feasibility, and repeatability.

Author

Widholm, Per, Ahlgren, André, Karlsson, Markus, Romu, Thobias, Tawil, Rabi, Wagner, Kathryn R., Statland, Jeffrey M., Wang, Leo H., Shieh, Perry B., van Engelen, Baziel G. M., Cadavid, Diego, Ronco, Lucienne, Odueyungbo, Adefowope O., Jiang, John G., Mellion, Michelle L., and Dahlqvist Leinhard, Olof

Abstract

Introduction/Aims: Functional performance tests are the gold standard to assess disease progression and treatment effects in neuromuscular disorders. These tests can be confounded by motivation, pain, fatigue, and learning effects, increasing variability and decreasing sensitivity to disease progression, limiting efficacy assessment in clinical trials with small sample sizes. We aimed to develop and validate a quantitative and objective method to measure skeletal muscle volume and fat content based on whole‐body fat‐referenced magnetic resonance imaging (MRI) for use in multisite clinical trials. Methods: Subjects aged 18 to 65 years, genetically confirmed facioscapulohumeral muscular dystrophy 1 (FSHD1), clinical severity 2 to 4 (Ricci's scale, range 0–5), were enrolled at six sites and imaged twice 4–12 weeks apart with T1‐weighted two‐point Dixon MRI covering the torso and upper and lower extremities. Thirty‐six muscles were volumetrically segmented using semi‐automatic multi‐atlas‐based segmentation. Muscle fat fraction (MFF), muscle fat infiltration (MFI), and lean muscle volume (LMV) were quantified for each muscle using fat‐referenced quantification. Results: Seventeen patients (mean age ± SD, 49.4 years ±13.02; 12 men) were enrolled. Within‐patient SD ranged from 1.00% to 3.51% for MFF and 0.40% to 1.48% for MFI in individual muscles. For LMV, coefficients of variation ranged from 2.7% to 11.7%. For the composite score average of all muscles, observed SDs were 0.70% and 0.32% for MFF and MFI, respectively; composite LMV coefficient of variation was 2.0%. Discussion: We developed and validated a method for measuring skeletal muscle volume and fat content for use in multisite clinical trials of neuromuscular disorders. [ABSTRACT FROM AUTHOR]

Published

2022

25. Brief assessment of cognitive function in myotonic dystrophy: Multicenter longitudinal study using computer‐assisted evaluation.

Author

Deutsch, Gayle K., Hagerman, Katharine A., Sampson, Jacinda, Dent, Gersham, Dekdebrun, Jeanne, Parker, Dana M., Thornton, Charles A., Heatwole, Chad R., Subramony, Sub H., Mankodi, Ami K., Ashizawa, Tetsuo, Statland, Jeffrey M., Arnold, W. David, Moxley, Richard T., and Day, John W.

Abstract

Introduction/Aims: Myotonic dystrophy type 1 (DM1) is known to affect cognitive function, but the best methods to assess central nervous system involvement in multicenter studies have not been determined. In this study our primary aim was to evaluate the potential of computerized cognitive tests to assess cognition in DM1. Methods: We conducted a prospective, longitudinal, observational study of 113 adults with DM1 at six sites. Psychomotor speed, attention, working memory, and executive functioning were assessed at baseline, 3 months, and 12 months using computerized cognitive tests. Results were compared with assessments of muscle function and patient reported outcomes (PROs), including the Myotonic Dystrophy Health Index (MDHI) and the 5‐dimension EuroQol (EQ‐5D‐5L) questionnaire. Results: Based on intraclass correlation coefficients, computerized cognitive tests had moderate to good reliability for psychomotor speed (0.76), attention (0.82), working memory speed (0.79), working memory accuracy (0.65), and executive functioning (0.87). Performance at baseline was lowest for working memory accuracy (P <.0001). Executive function performance improved from baseline to 3 months (P <.0001), without further changes over 1 year. There was a moderate correlation between poorer executive function and larger CTG repeat size (r = −0.433). There were some weak associations between PROs and cognitive performance. Discussion: Computerized tests of cognition are feasible in multicenter studies of DM1. Poor performance was exhibited in working memory, which may be a useful variable in clinical trials. Learning effects may have contributed to the improvement in executive functioning. The relationship between PROs and cognitive impairment in DM1 requires further study. [ABSTRACT FROM AUTHOR]

Published

2022

26. Muscarinic receptor activation tunes mouse stratum oriens interneurones to amplify spike reliability.

Author

Lawrence, J. Josh, Grinspan, Zachary M., Statland, Jeffrey M., and McBain, Chris J.

Subjects

*CHOLINERGIC mechanisms, *HIPPOCAMPUS (Brain), *NEURAL circuitry, *NEURONS, *MUSCARINIC receptors

Abstract

Cholinergic activation of hippocampal targets can initiate and sustain network oscillations in vivo and in vitro, yet the impact of cholinergic modulation on the oscillatory properties of interneurones remains virtually unexplored. Using whole cell current clamp recordings in acute hippocampal slices, we investigated the influence of muscarinic receptor (mAChR) activation on the oscillatory properties of CA1 stratum oriens (SO) interneurones in vitro. In response to suprathreshold oscillatory input, mAChR activation increased spike reliability and precision, and extended the bandwidth that interneurone firing phase-locked. These suprathreshold effects were largest at theta frequencies, indicating that mAChR activation tunes active conductances to enhance firing reliability and precision to theta frequency input. Muscarinic tuning of the intrinsic oscillatory properties of interneurones is a novel mechanism that may be crucial for the genesis of the theta rhythm. [ABSTRACT FROM AUTHOR]

Published

2006

27. Predictors of functional outcomes in patients with facioscapulohumeral muscular dystrophy.

Author

Katz, Natalie K, Hogan, John, Delbango, Ryan, Cernik, Colin, Tawil, Rabi, and Statland, Jeffrey M

Subjects

*SUPERVISED learning, *FACIOSCAPULOHUMERAL muscular dystrophy, *PROPORTIONAL hazards models, *MUSCULAR dystrophy, *FUNCTIONAL status, *DISEASE duration, *DISEASE progression, *RESEARCH, *RESEARCH methodology, *PROGNOSIS, *EVALUATION research, *COMPARATIVE studies, *RESEARCH funding, *LONGITUDINAL method

Abstract

Facioscapulohumeral muscular dystrophy (FSHD) is one of the most prevalent muscular dystrophies characterized by considerable variability in severity, rates of progression and functional outcomes. Few studies follow FSHD cohorts long enough to understand predictors of disease progression and functional outcomes, creating gaps in our understanding, which impacts clinical care and the design of clinical trials. Efforts to identify molecularly targeted therapies create a need to better understand disease characteristics with predictive value to help refine clinical trial strategies and understand trial outcomes. Here we analysed a prospective cohort from a large, longitudinally followed registry of patients with FSHD in the USA to determine predictors of outcomes such as need for wheelchair use. This study analysed de-identified data from 578 individuals with confirmed FSHD type 1 enrolled in the United States National Registry for FSHD Patients and Family members. Data were collected from January 2002 to September 2019 and included an average of 9 years (range 0-18) of follow-up surveys. Data were analysed using descriptive epidemiological techniques, and risk of wheelchair use was determined using Cox proportional hazards models. Supervised machine learning analysis was completed using Random Forest modelling and included all 189 unique features collected from registry questionnaires. A separate medications-only model was created that included 359 unique medications reported by participants. Here we show that smaller allele sizes were predictive of earlier age at onset, diagnosis and likelihood of wheelchair use. Additionally, we show that females were more likely overall to progress to wheelchair use and at a faster rate as compared to males, independent of genetics. Use of machine learning models that included all reported clinical features showed that the effect of allele size on progression to wheelchair use is small compared to disease duration, which may be important to consider in trial design. Medical comorbidities and medication use add to the risk for need for wheelchair dependence, raising the possibility for better medical management impacting outcomes in FSHD. The findings in this study will require further validation in additional, larger datasets but could have implications for clinical care, and inclusion criteria for future clinical trials in FSHD. [ABSTRACT FROM AUTHOR]

Published

2021

28. A double-blind, placebo-controlled, randomized trial of PXT3003 for the treatment of Charcot-Marie-Tooth type 1A.

Author

Attarian, Shahram, Young, Peter, Brannagan, Thomas H., Adams, David, Van Damme, Philip, Thomas, Florian P., Casanovas, Carlos, Tard, Céline, Walter, Maggie C., Péréon, Yann, Walk, David, Stino, Amro, de Visser, Marianne, Verhamme, Camiel, Amato, Anthony, Carter, Gregory, Magy, Laurent, Statland, Jeffrey M., and Felice, Kevin

Subjects

*NEUROMUSCULAR diseases, *CHARCOT-Marie-Tooth disease, *MISSING data (Statistics), *TREATMENT effectiveness, *SENSITIVITY analysis

Abstract

Background: Charcot-Marie-Tooth disease type 1A (CMT1A) is a rare, orphan, hereditary neuromuscular disorder with no cure and for which only symptomatic treatment is currently available. A previous phase 2 trial has shown preliminary evidence of efficacy for PXT3003 in treating CMT1A. This phase 3, international, randomized, double-blind, placebo-controlled study further investigated the efficacy and safety of high- or low-dose PXT3003 (baclofen/naltrexone/D-sorbitol [mg]: 6/0.70/210 or 3/0.35/105) in treating subjects with mild to moderate CMT1A.Methods: In this study, 323 subjects with mild-to-moderate CMT1A were randomly assigned in a 1:1:1 ratio to receive 5 mL of high- or low-dose PXT3003, or placebo, orally twice daily for up to 15 months. Efficacy was assessed using the change in Overall Neuropathy Limitations Scale total score from baseline to months 12 and 15 (primary endpoint). Secondary endpoints included the 10-m walk test and other assessments. The high-dose group was discontinued early due to unexpected crystal formation in the high-dose formulation, which resulted in an unanticipated high discontinuation rate, overall and especially in the high-dose group. The statistical analysis plan was adapted to account for the large amount of missing data before database lock, and a modified full analysis set was used in the main analyses. Two sensitivity analyses were performed to check the interpretation based on the use of the modified full analysis set.Results: High-dose PXT3003 demonstrated significant improvement in the Overall Neuropathy Limitations Scale total score vs placebo (mean difference: - 0.37 points; 97.5% CI [- 0.68 to - 0.06]; p = 0.008), and consistent treatment effects were shown in the sensitivity analyses. Both PXT3003 doses were safe and well-tolerated.Conclusion: The high-dose group demonstrated a statistically significant improvement in the primary endpoint and a good safety profile. Overall, high-dose PXT3003 is a promising treatment option for patients with Charcot-Marie-Tooth disease type 1A. [ABSTRACT FROM AUTHOR]

Published

2021

29. Long‐term efficacy and safety of dichlorphenamide for treatment of primary periodic paralysis.

Author

Sansone, Valeria A., Johnson, Nicholas E., Hanna, Michael G., Ciafaloni, Emma, Statland, Jeffrey M., Shieh, Perry B., Cohen, Fredric, and Griggs, Robert C.

Abstract

Introduction/Aim: Long‐term efficacy and safety of dichlorphenamide (DCP) were characterized in patients with primary periodic paralysis (PPP). Methods: Patients with PPP in a double‐blind, placebo‐controlled study were randomly assigned to receive DCP 50 mg twice daily or placebo for 9 weeks, followed by a 52‐week open‐label DCP treatment phase (DCP/DCP and placebo/DCP populations). Efficacy (attack rate, severity‐weighted attack rate) and safety were assessed in patients completing the study (61 weeks). In this post hoc analysis, efficacy and safety data were pooled from hyperkalemic and hypokalemic substudies. Results: Sixty‐three adults (age, 19‐76 years) completed the double‐blind phase; 47 (74.6%) of these patients completed 61 weeks. There were median decreases in weekly attack and severity‐weighted attack rates from baseline to week 61 (DCP/DCP [n = 25], −1.00 [P <.0001]; placebo/DCP [n = 20], −0.63 [P =.01] and DCP/DCP, −2.25 [P <.0001]; placebo/DCP, −1.69 [P =.01]). Relatively smaller median decreases in weekly attack and severity‐weighted attack rates occurred from weeks 9 to 61 among patients receiving DCP continuously (n = 26; −0.14 [P =.1] and −0.24 [P =.09]) than among those switching from placebo to DCP after 9 weeks (n = 16; −1.04 [P =.049] and −2.72 [P =.08]). Common adverse events (AEs) were paresthesia and cognition‐related events, which typically first occurred within 1 month of blinded treatment initiation and in rare cases led to treatment discontinuation. Dose reductions were frequently associated with common AE resolution. Discussion: One‐year open‐label DCP treatment after a 9‐week randomized, controlled study confirmed long‐term DCP remains safe and effective for chronic use. Tolerability issues (paresthesia, cognition‐related AEs) were manageable in most patients. [ABSTRACT FROM AUTHOR]

Published

2021

30. The facioscapulohumeral muscular dystrophy Rasch‐built overall disability scale (FSHD‐RODS).

Author

Mul, Karlien, Hamadeh, Tatiana, Horlings, Corinne G. C., Tawil, Rabi, Statland, Jeffrey M., Sacconi, Sabrina, Corbett, Alastair J., Voermans, Nicol C., Faber, Catharina G., Engelen, Baziel G. M., and Merkies, Ingemar S. J.

Subjects

*FACIOSCAPULOHUMERAL muscular dystrophy, *DISABILITIES, *RASCH models, *GENETIC disorders, *STATISTICAL reliability, *PEOPLE with disabilities

Abstract

Background and objectives: Facioscapulohumeral muscular dystrophy (FHSD) is a debilitating inherited muscle disease for which various therapeutic strategies are being investigated. Thus far, little attention has been given in FSHD to the development of scientifically sound outcome measures fulfilling regulatory authority requirements. The aim of this study was to design a patient‐reported Rasch‐built interval scale on activity and participation for FSHD. Methods: A pre‐phase FSHD‐Rasch‐built overall disability scale (pre‐FSHD‐RODS; consisting of 159 activity/participation items), based on the World Health Organization international classification of disease‐related functional consequences was completed by 762 FSHD patients (Netherlands: n = 171; UK: n = 287; United States: n = 221; France: n = 52; Australia: n = 32). A proportion of the patient cohort completed it twice (n = 230; interval 2–4 weeks; reliability studies). The pre‐FSHD‐RODS was subjected to Rasch analyses to create a model fulfilling its requirements. Validity studies were performed through correlation with the motor function measure. Results: The pre‐FSHD‐RODS did not meet the Rasch model expectations. Based on determinants such as misfit statistics and misfit residuals, differential item functioning, and local dependency, we systematically removed items until a final 38‐inquiry (originating from 32 items; six items split) FSHD‐RODS was constructed achieving Rasch model expectations. Adequate test‐retest reliability and (cross‐cultural and external) validity scores were obtained. Conclusions: The FSHD‐RODS is a disease‐specific interval measure suitable for detecting activity and participation restrictions in patients with FSHD with good item/person reliability and validity scores. The use of this scale is recommended in the near future, to determine the functional deterioration slope in FSHD per year as a preparation for the upcoming clinical intervention trials in FSHD. [ABSTRACT FROM AUTHOR]

Published

2021

31. The clinical spectrum of primary lateral sclerosis.

Author

Barohn, Richard J., Fink, John K., Heiman-Patterson, Terry, Huey, Edward D., Murphy, Jennifer, Statland, Jeffrey M., Turner, Martin R., and Elman, Lauren

Abstract

Primary lateral sclerosis is a distinct entity that has recently been classified as a “restricted phenotype” of ALS. It is characterized by a pattern of isolated upper motor neuron involvement that often begins in the legs and spreads diffusely. Distinction from other conditions requires careful consideration of clinical presentation and time course of disease. Mills’ Syndrome is a rare unilateral variant of primary lateral sclerosis. Cognitive and behavioral involvement may occur. [ABSTRACT FROM AUTHOR]

Published

2020

32. Guidelines on clinical presentation and management of nondystrophic myotonias.

Author

Stunnenberg, Bas C., LoRusso, Samantha, Arnold, W. David, Barohn, Richard J., Cannon, Stephen C., Fontaine, Bertrand, Griggs, Robert C., Hanna, Michael G., Matthews, Emma, Meola, Giovanni, Sansone, Valeria A., Trivedi, Jaya R., van Engelen, Baziel G.M., Vicart, Savine, and Statland, Jeffrey M.

Abstract

The nondystrophic myotonias are rare muscle hyperexcitability disorders caused by gain-of-function mutations in the SCN4A gene or loss-of-function mutations in the CLCN1 gene. Clinically, they are characterized by myotonia, defined as delayed muscle relaxation after voluntary contraction, which leads to symptoms of muscle stiffness, pain, fatigue, and weakness. Diagnosis is based on history and examination findings, the presence of electrical myotonia on electromyography, and genetic confirmation. In the absence of genetic confirmation, the diagnosis is supported by detailed electrophysiological testing, exclusion of other related disorders, and analysis of a variant of uncertain significance if present. Symptomatic treatment with a sodium channel blocker, such as mexiletine, is usually the first step in management, as well as educating patients about potential anesthetic complications. [ABSTRACT FROM AUTHOR]

Published

2020

33. Magnetic resonance imaging correlates with electrical impedance myography in facioscapulohumeral muscular dystrophy.

Author

Hamel, Johanna, Lee, Phil, Glenn, Melanie D., Burka, Tekalign, Choi, In‐Young, Friedman, Seth D., Shaw, Dennis W. W., McCalley, Ayla, Herbelin, Laura, Dimachkie, Mazen M., Lemmers, Richard, Maarel, Silvère M., Barohn, Richard J., Tawil, Rabi, Statland, Jeffrey M., Choi, In-Young, and van der Maarel, Silvère M

Subjects

*MUSCULAR dystrophy, *ELECTRODIAGNOSIS, *RESEARCH, *SKELETAL muscle, *MUSCLES, *ANTHROPOMETRY, *RESEARCH methodology, *MAGNETIC resonance imaging, *EVALUATION research, *MEDICAL cooperation, *COMPARATIVE studies, *QUADRICEPS muscle, *DIAGNOSIS, *BIOELECTRIC impedance, *RESEARCH funding, *ADIPOSE tissues

Abstract

Introduction: Electrical impedance myography (EIM) has been proposed as a noninvasive biomarker of muscle composition in facioscapulohumeral muscular dystrophy (FSHD). Here we determine the associations of EIM variables with muscle structure measured by MRI.Methods: We evaluated 20 patients with FSHD at two centers, comparing EIM measurements (resistance, reactance, and phase at 50, 100, and 211 kHZ) recorded from bilateral vastus lateralis, tibialis anterior, and medial gastrocnemius muscles to MRI skin and subcutaneous fat thickness, MRI T1-based muscle severity score (T1 muscle score), and MRI quantitative intramuscular Dixon fat fraction (FF).Results: While reactance and phase both correlated with FF and T1 muscle score, 50 kHz reactance was most sensitive to muscle structure alterations measured by both T1 score (ρ = -0.71, P < .001) and FF (ρ = -0.74, P < .001).Discussion: This study establishes the correlation of EIM with structural MRI features in FSHD and supports further evaluation of EIM as a potential biomarker in FSHD clinical trials. [ABSTRACT FROM AUTHOR]

Published

2020

34. Limb-girdle muscular dystrophy: A perspective from adult patients on what matters most.

Author

Hunter, Michael, Heatwole, Chad, Wicklund, Matthew, Weihl, Conrad C., Mozaffar, Tahseen, Statland, Jeffrey M., and Johnson, Nicholas E.

Abstract

Introduction: Limb-girdle muscular dystrophy (LGMD) consists of over 30 genetic conditions with varying clinical phenotypes primarily affecting pelvic girdle, shoulder girdle, and other proximal limb muscles. Studies focusing on the physical, mental, and social effects of this disease from the patient's perspective are limited.Methods: Adults with LGMD were interviewed and asked to identify issues that have the greatest impact on their quality of life. Each interview was recorded, transcribed, coded, and analyzed.Results: Participants provided 1385 direct quotes. One hundred sixty-five potential symptoms of importance were identified and grouped into 15 larger themes. The most frequently reported themes included limitations with mobility, difficulty performing activities, social role limitations, and emotional distress.Discussion: There are multiple symptoms that alter the lives of adults with LGMD. These affect their physical, emotional, and social health, and may be amenable to medical intervention. [ABSTRACT FROM AUTHOR]

Published

2019

35. Effect of Mexiletine on Muscle Stiffness in Patients With Nondystrophic Myotonia Evaluated Using Aggregated N-of-1 Trials.

Author

Stunnenberg, Bas C., Raaphorst, Joost, Groenewoud, Hans M., Statland, Jeffrey M., Griggs, Robert C., Woertman, Willem, Stegeman, Dick F., Timmermans, Janneke, Trivedi, Jaya, Matthews, Emma, Saris, Christiaan G. J., Schouwenberg, Bas J., Drost, Gea, van Engelen, Baziel G. M., and van der Wilt, Gert Jan

Subjects

*CLINICAL trials, *COMPARATIVE studies, *RESEARCH methodology, *MEDICAL cooperation, *MEXILETINE, *MYOTONIA, *PROBABILITY theory, *RESEARCH, *SYMPTOMS, *EVALUATION research, *BLIND experiment, *SODIUM channel blockers, *STATISTICAL models, *THERAPEUTICS

Abstract

Importance: In rare diseases it is difficult to achieve high-quality evidence of treatment efficacy because of small cohorts and clinical heterogeneity. With emerging treatments for rare diseases, innovative trial designs are needed.Objective: To investigate the effectiveness of mexiletine in nondystrophic myotonia using an aggregated N-of-1 trials design and compare results between this innovative design and a previously conducted RCT.Design, Setting, and Participants: A series of aggregated, double-blind, randomized, placebo-controlled N-of-1-trials, performed in a single academic referral center. Thirty Dutch adult patients with genetically confirmed nondystrophic myotonia (38 patients screened) were enrolled between February 2014 and June 2015. Follow-up was completed in September 2016.Interventions: Mexiletine (600 mg daily) vs placebo during multiple treatment periods of 4 weeks.Main Outcomes and Measures: Reduction in daily-reported muscle stiffness on a scale of 1 to 9, with higher scores indicating more impairment. A Bayesian hierarchical model aggregated individual N-of-1 trial data to determine the posterior probability of reaching a clinically meaningful effect of a greater than 0.75-point difference.Results: Among 30 enrolled patients (mean age, 43.4 [SD, 15.24] years; 22% men; 19 CLCN1 and 11 SCN4A genotype), 27 completed the study and 3 dropped out (1 because of a serious adverse event). In 24 of the 27 completers, a clinically meaningful treatment effect was found. In the Bayesian hierarchical model, mexiletine resulted in a 100% posterior probability of reaching a clinically meaningful reduction in self-reported muscle stiffness for the nondystrophic myotonia group overall and the CLCN1 genotype subgroup and 93% posterior probability for the SCN4A genotype subgroup. In the total nondystrophic myotonia group, the median muscle stiffness score was 6.08 (interquartile range, 4.71-6.80) at baseline and was 2.50 (95% credible interval [CrI], 1.77-3.24) during the mexiletine period and 5.56 (95% CrI, 4.73-6.39) during the placebo period; difference in symptom score reduction, 3.06 (95% CrI, 1.96-4.15; n = 27) favoring mexiletine. The most common adverse event was gastrointestinal discomfort (21 mexiletine [70%], 1 placebo [3%]). One serious adverse event occurred (1 mexiletine [3%]; allergic skin reaction). Using frequentist reanalysis, mexiletine compared with placebo resulted in a mean reduction in daily-reported muscle stiffness of 3.12 (95% CI, 2.46-3.78), consistent with the previous RCT treatment effect of 2.69 (95% CI, 2.12-3.26).Conclusions and Relevance: In a series of N-of-1 trials of mexiletine vs placebo in patients with nondystrophic myotonia, there was a reduction in mean daily-reported muscle stiffness that was consistent with the treatment effect in a previous randomized clinical trial. These findings support the efficacy of mexiletine for treatment of nondystrophic myotonia as well as the feasibility of N-of-1 trials for assessing interventions in some chronic rare diseases.Trial Registration: ClinicalTrials.gov Identifier: NCT02045667. [ABSTRACT FROM AUTHOR]

Published

2018

36. Electrical impedance myography in facioscapulohumeral muscular dystrophy: A 1-year follow-up study.

Author

Mul, Karlien, Heatwole, Chad, Eichinger, Katy, Dilek, Nuran, Martens, William B., Van Engelen, Baziel G. M., Tawil, Rabi, and Statland, Jeffrey M.

Subjects

*MUSCULAR dystrophy diagnosis, *ELECTROMYOGRAPHY, *LONGITUDINAL method, *MUSCLE strength, *TREATMENT effectiveness, *PREDICTIVE tests, *DISEASE progression, RESEARCH evaluation

Abstract

Introduction: Electrical impedance myography (EIM) is a noninvasive technique for measuring muscle composition and a potential physiological biomarker for facioscapulohumeral muscular dystrophy (FSHD).Methods: Thirty-two participants with genetically confirmed and clinically affected FSHD underwent EIM in 7 muscles bilaterally. Correlations between EIM and baseline clinical measures were used to select EIM variables of interest in FSHD, and EIM and clinical measures were followed for 1 year.Results: There were no significant changes in the EIM variables. Although 50-kHZ reactance correlated the strongest with clinical measures at baseline, the 50-211-kHZ phase ratio demonstrated lower within-subject 12-month variability, potentially offering sample size savings for FSHD clinical trial planning.Discussion: EIM did not identify significant disease progression over 12 months. It is currently unclear whether this is because of limitations of the technology or the slow rate of disease progression in this cohort of FSHD patients over this period of time. Muscle Nerve 58: 213-218, 2018. [ABSTRACT FROM AUTHOR]

Published

2018

37. Facioscapulohumeral muscular dystrophy functional composite outcome measure.

Author

Eichinger, Katy, Heatwole, Chad, Iyadurai, Stanley, King, Wendy, Baker, Lindsay, Heininger, Susanne, Bartlett, Amy, Dilek, Nuran, Martens, William B., Mcdermott, Michael, Kissel, John T., Tawil, Rabi, and Statland, Jeffrey M.

Abstract

Introduction: We developed an evaluator-administered functional facioscapulohumeral muscular dystrophy composite outcome measure (FSHD-COM) comprising patient-identified areas of functional burden for future clinical trials.Methods: We performed a prospective observational study of 41 patients with FSHD at 2 sites. The FSHD-COM includes functional assessment of the legs, shoulders and arms, trunk, hands, and balance/mobility. We determined the test-retest reliability and convergent validity compared to established FSHD disease metrics.Results: The FSHD-COM demonstrated excellent test-retest reliability (intraclass correlation coefficient [ICC] 0.96; subscale ICC range, 0.90-0.94). Cross-sectional associations between the FSHD-COM and disease duration, clinical severity, and strength were moderate to strong (Pearson correlation coefficient range |0.51-0.92|).Discussion: The FSHD-COM is a disease-relevant, functional composite outcome measure suitable for future FSHD clinical trials that shows excellent test-retest reliability and cross-sectional associations to disease measures. Future directions include determining multisite reliability, sensitivity to change, and the minimal clinically important change in the FSHD-COM. Muscle Nerve, 2018. [ABSTRACT FROM AUTHOR]

Published

2018

38. Reply: Wheelchair use in genetically confirmed FSHD1 from a large cohort study in Chinese population.

Author

Katz, Natalie K, Hogan, John, Delbango, Ryan, Cernik, Colin, Tawil, Rabi, and Statland, Jeffrey M

Subjects

*WHEELCHAIRS, *MUSCULAR dystrophy, *LONGITUDINAL method

Published

2022

39. Validity of the 6 minute walk test in facioscapulohumeral muscular dystrophy.

Author

Eichinger, Katy, Heatwole, Chad, Heininger, Susanne, Stinson, Nikia, Matichak Stock, Carly, Grosmann, Carla, Wagner, Kathryn R., Tawil, Rabi, Statland, Jeffrey M., and FSHD Clinical Trials Research Network

Subjects

*MUSCULAR dystrophy diagnosis, *COMPARATIVE studies, *LONGITUDINAL method, *RESEARCH methodology, *MEDICAL cooperation, *MUSCLE strength, *MUSCULAR dystrophy, *RESEARCH, *RESEARCH funding, *WALKING, *EVALUATION research, *CROSS-sectional method, *RETROSPECTIVE studies, *SEVERITY of illness index, RESEARCH evaluation

Abstract

Introduction: In preparation for future clinical trials, we determined the reliability, relationship to measures of disease severity, and consistency across sites of the 6 Minute Walk Test (6MWT) in patients with facioscapulohumeral muscular dystrophy (FSHD).Methods: Genetically defined and clinically affected FSHD participants at 2 sites performed the 6MWT, the Timed Up and Go, and the 30 foot Go/Timed 10 meter test as measures of mobility using standard procedures.Results: Eight-six participants representing the full range of severity performed the 6MWT. The mean 6MWT distance was 404.3 meters (SD 123.9), with no difference between sites. The 6MWT was reliable (n = 25; intraclass correlation coefficient = 0.99) and demonstrated moderate to strong correlations with lower extremity strength, functional outcomes, and FSHD Clinical Score.Conclusions: The 6MWT is reliable and is associated with other measures of FSHD disease severity. Future directions include assessing its sensitivity to disease progression. Muscle Nerve 55: 333-337, 2017. [ABSTRACT FROM AUTHOR]

Published

2017

40. Combined N-of-1 trials to investigate mexiletine in non-dystrophic myotonia using a Bayesian approach; study rationale and protocol.

Author

Stunnenberg, Bas C., Woertman, Willem, Raaphorst, Joost, Statland, Jeffrey M., Griggs, Robert C., Timmermans, Janneke, Saris, Christiaan G., Schouwenberg, Bas J., Groenewoud, Hans M., Stegeman, Dick F., van Engelen, Baziel G. M., Drost, Gea, and van der Wilt, Gert Jan

Subjects

*MYOTONIA, *MEXILETINE, *BAYESIAN analysis, *MUSCLE diseases

Abstract

Background: To obtain evidence for the clinical and cost-effectiveness of treatments for patients with rare diseases is a challenge. Non-dystrophic myotonia (NDM) is a group of inherited, rare muscle diseases characterized by muscle stiffness. The reimbursement of mexiletine, the expert opinion drug for NDM, has been discontinued in some countries due to a lack of independent randomized controlled trials (RCTs). It remains unclear however, which concessions can be accepted towards the level 1 evidence needed for coverage decisions, in rare diseases. Considering the large number of rare diseases with a lack of treatment evidence, more experience with innovative trial designs is needed. Both NDM and mexiletine are well suited for an N-of-1 trial design. A Bayesian approach allows for the combination of N-of-1 trials, which enables the assessment of outcomes on the patient and group level simultaneously. Methods/Design: We will combine 30 individual, double-blind, randomized, placebo-controlled N-of-1 trials of mexiletine (600 mg daily) vs. placebo in genetically confirmed NDM patients using hierarchical Bayesian modeling. Our results will be compared and combined with the main results of an international cross-over RCT (mexiletine vs. placebo in NDM) published in 2012 that will be used as an informative prior. Similar criteria of eligibility, treatment regimen, end-points and measurement instruments are employed as used in the international cross-over RCT. Discussion: The treatment of patients with NDM with mexiletine offers a unique opportunity to compare outcomes and efficiency of novel N-of-1 trial-based designs and conventional approaches in producing evidence of clinical and cost-effectiveness of treatments for patients with rare diseases. Trial registration: ClinicalTrials.gov Identifier: NCT02045667 [ABSTRACT FROM AUTHOR]

Published

2015

41. Phenotypic diversity in an international Cure VCP Disease registry.

Author

Ikenaga, Chiseko, Findlay, Andrew R., Seiffert, Michelle, Peck, Allison, Peck, Nathan, Johnson, Nicholas E., Statland, Jeffrey M., and Weihl, Conrad C.

Subjects

*MEDICAL registries, *OSTEITIS deformans, *AMYOTROPHIC lateral sclerosis, *BONE morphogenetic protein receptors, *GENETIC mutation, *STAIR climbing

Abstract

Background: Dominant mutations in valosin-containing protein (VCP) gene cause an adult onset inclusion body myopathy, Paget's disease of bone, and frontotemporal dementia also termed multisystem proteinopathy (MSP). The genotype-phenotype relationships in VCP-related MSP are still being defined; in order to understand this better, we investigated the phenotypic diversity and patterns of weakness in the Cure VCP Disease Patient Registry.Methods: Cure VCP Disease, Inc. was founded in 2018 for the purpose of connecting patients with VCP gene mutations and researchers to help advance treatments and cures. Cure VCP Disease Patient Registry is maintained by Coordination of Rare Diseases at Sanford. The results of two questionnaires with a 5-point Likert scale questions regarding to patients' disease onset, symptoms, and daily life were obtained from 59 participants (28 males and 31 females) between June 2018 and May 2020. Independent of the registry, 22 patients were examined at the Cure VCP Disease annual patient conference in 2019.Results: In the questionnaires of the registry, fifty-three patients (90%) reported that they were with inclusion body myopathy, 17 patients (29%) with Paget's disease of bone, eight patients (14%) with dementia, two patients (3%) with amyotrophic lateral sclerosis, and a patient with parkinsonism. Thirteen patients (22%) reported dysphagia and 25 patients (42%) reported dyspnea on exertion. A self-reported functional rating scale for motor function identified challenges with sit to stand (72%), walking (67%), and climbing stairs (85%). Thirty-five (59%) patients in the registry answered that their quality of life is more than good. As for the weakness pattern of the 22 patients who were evaluated at the Cure VCP Disease annual conference, 50% of patients had facial weakness, 55% had scapular winging, 68% had upper proximal weakness, 41% had upper distal weakness, 77% had lower proximal, and 64% had lower distal weakness.Conclusions: The Cure VCP Disease Patient Registry is useful for deepening the understanding of patient daily life, which would be a basis to develop appropriate clinical outcome measures. The registry data is consistent with previous studies evaluating VCP patients in the clinical setting. Patient advocacy groups are essential in developing and maintaining disease registries. [ABSTRACT FROM AUTHOR]

Published

2020

42. Clinical trial readiness to solve barriers to drug development in FSHD (ReSolve): protocol of a large, international, multi-center prospective study.

Author

LoRusso, Samantha, Johnson, Nicholas E., McDermott, Michael P., Eichinger, Katy, Butterfield, Russell J., Carraro, Elena, Higgs, Kiley, Lewis, Leann, Mul, Karlien, Sacconi, Sabrina, Sansone, Valeria A., Shieh, Perry, van Engelen, Baziel, Wagner, Kathryn, Wang, Leo, Statland, Jeffrey M., Tawil, Rabi, and ReSolve Investigators and the FSHD CTRN18

Subjects

*FACIOSCAPULOHUMERAL muscular dystrophy, *LONGITUDINAL method, *DRUG development, *CLINICAL trials, *DUAL-energy X-ray absorptiometry, *MUSCULAR dystrophy

Abstract

Background: Facioscapulohumeral muscular dystrophy (FSHD) is a dominantly-inherited progressive muscular dystrophy caused by de-repression of the DUX4 gene, which causes disease by a toxic-gain-of-function. As molecularly targeted drugs move from preclinical testing into human trials, it is essential that we validate clinical trial tools and methodology to facilitate the drug development process.Methods/design: The primary goal of this study is to hasten drug development for FSHD by validating two novel clinical outcome assessments (COAs) and refining clinical trial strategies. We will perform an 18-month longitudinal study in 220 genetically confirmed and clinically affected participants using our FSHD Clinical Trial Research Network, comprised of 8 sites in the United States, and 3 collaborating sites in Europe. Visits occur at baseline and months 3, 12, and 18. At each visit we will collect: 1) a novel FSHD functional composite COA made up of 18 evaluator-administered motor tasks in the domains of shoulder/arm, hand, core/abdominal, leg, and balance function; and 2) electrical impedance myography as a novel muscle quality biomarker (US sites). Other COAs include 1) Domain 1 of the Motor Function Measure; 2) Reachable workspace; 3) orofacial strength using the Iowa Oral Performance Instrument; 4) lean muscle mass using dual-energy X-ray absorptiometry (DEXA); 5) strength as measured by quantitative myometry and manual muscle testing; and 6) the FSHD Health Index and other patient-reported outcomes. Plasma, DNA, RNA, and serum will be collected for future biomarker studies. We will use an industry standard multi-site training plan. We will evaluate the test-retest reliability, validity, and sensitivity to disease progression, and minimal clinically important changes of our new COAs. We will assess associations between demographic and genetic factors and the rate of disease progression to inform refinement of eligibility criteria for future clinical trials.Discussion: To the best of our knowledge, this is the largest collaborative study of patients with FSHD performed in the US and Europe. The results of this study will enable more efficient clinical trial design. During the conduct of the study, relevant data will be made available for investigators or companies pursuing novel FSHD therapeutics.Trial Registration: clinicaltrials.gov NCT03458832; Date of registration: 1/11/2018. [ABSTRACT FROM AUTHOR]

Published

2019

43. Using automated electronic medical record data extraction to model ALS survival and progression.

Author

Karanevich, Alex G, Weisbrod, Luke J, Jawdat, Omar, Barohn, Richard J, Gajewski, Byron J, He, Jianghua, and Statland, Jeffrey M

Subjects

*ELECTRONIC health records, *AMYOTROPHIC lateral sclerosis, *DISEASE progression, *PROPORTIONAL hazards models, *PREDICTION models, *BODY mass index, *REGRESSION analysis

Abstract

Background: To assess the feasibility of using automated capture of Electronic Medical Record (EMR) data to build predictive models for amyotrophic lateral sclerosis (ALS) outcomes.Methods: We used an Informatics for Integrating Biology and the Bedside search discovery tool to identify and extract data from 354 ALS patients from the University of Kansas Medical Center EMR. The completeness and integrity of the data extraction were verified by manual chart review. A linear mixed model was used to model disease progression. Cox proportional hazards models were used to investigate the effects of BMI, gender, and age on survival.Results: Data extracted from the EMR was sufficient to create simple models of disease progression and survival. Several key variables of interest were unavailable without including a manual chart review. The average ALS Functional Rating Scale - Revised (ALSFRS-R) baseline score at first clinical visit was 34.08, and average decline was - 0.64 per month. Median survival was 27 months after first visit. Higher baseline ALSFRS-R score and BMI were associated with improved survival, higher baseline age was associated with decreased survival.Conclusions: This study serves to show that EMR-captured data can be extracted and used to track outcomes in an ALS clinic setting, potentially important for post-marketing research of new drugs, or as historical controls for future studies. However, as automated EMR-based data extraction becomes more widely used there will be a need to standardize ALS data elements and clinical forms for data capture so data can be pooled across academic centers. [ABSTRACT FROM AUTHOR]

Published

2018

44. Combined N-of-1 trials to investigate mexiletine in non-dystrophic myotonia using a Bayesian approach; study rationale and protocol.

Author

Stunnenberg, Bas C, Woertman, Willem, Raaphorst, Joost, Statland, Jeffrey M, Griggs, Robert C, Timmermans, Janneke, Saris, Christiaan G, Schouwenberg, Bas J, Groenewoud, Hans M, Stegeman, Dick F, van Engelen, Baziel G M, Drost, Gea, and van der Wilt, Gert Jan

Abstract

Background: To obtain evidence for the clinical and cost-effectiveness of treatments for patients with rare diseases is a challenge. Non-dystrophic myotonia (NDM) is a group of inherited, rare muscle diseases characterized by muscle stiffness. The reimbursement of mexiletine, the expert opinion drug for NDM, has been discontinued in some countries due to a lack of independent randomized controlled trials (RCTs). It remains unclear however, which concessions can be accepted towards the level 1 evidence needed for coverage decisions, in rare diseases. Considering the large number of rare diseases with a lack of treatment evidence, more experience with innovative trial designs is needed. Both NDM and mexiletine are well suited for an N-of-1 trial design. A Bayesian approach allows for the combination of N-of-1 trials, which enables the assessment of outcomes on the patient and group level simultaneously.Methods/design: We will combine 30 individual, double-blind, randomized, placebo-controlled N-of-1 trials of mexiletine (600 mg daily) vs. placebo in genetically confirmed NDM patients using hierarchical Bayesian modeling. Our results will be compared and combined with the main results of an international cross-over RCT (mexiletine vs. placebo in NDM) published in 2012 that will be used as an informative prior. Similar criteria of eligibility, treatment regimen, end-points and measurement instruments are employed as used in the international cross-over RCT.Discussion: The treatment of patients with NDM with mexiletine offers a unique opportunity to compare outcomes and efficiency of novel N-of-1 trial-based designs and conventional approaches in producing evidence of clinical and cost-effectiveness of treatments for patients with rare diseases.Trial Registration: ClinicalTrials.gov Identifier: NCT02045667. [ABSTRACT FROM AUTHOR]

Published

2015

45. Somatodendritic Kv7/KCNQ/M Channels Control Interspike Interval in Hippocampal Interneurons.

Author

Lawrence, J. Josh, Saraga, Fernanda, Churchill, Joseph F., Statland, Jeffrey M., Travis, Katherine E., Skinner, Frances K., and McBain, Chris J.

Subjects

*POTASSIUM channels, *HIPPOCAMPUS (Brain), *ELECTRIC stimulation, *NEURONS, *CELLS

Abstract

The M-current (IM), comprised of Kv7 channels, is a voltage-activated K+ conductance that plays a key role in the control of cell excitability. In hippocampal principal cells, IM controls action potential (AP) accommodation and contributes to the medium-duration after hyperpolarization, but the role of IM in control of interneuron excitability remains unclear. Here, we investigated IM in hippocampal stratum oriens (SO) interneurons, both from wild-type and transgenic mice in which green fluorescent protein (GFP) was expressed in somatostatin-containing interneurons. Somatodendritic expression of Kv7.2 or Kv7.3 subunits was colocalized in a subset of GFP+ SO interneurons, corresponding to oriens-lacunosum moleculare (O-LM) cells. Under voltage clamp (VC) conditions at -30 mV, the Kv7 channel antagonists linopirdine/XE-991 abolished the IM amplitude present during relaxation from -30 to -50mV and reduced the holding current (Ihold ). In addition, 0.5mM tetraethylammonium reduced IM, suggesting that IM was composed of Kv7.2-containing channels. In contrast, the Kv7 channel opener retigabine increased IM amplitude and Ihold. When strongly depolarized in VC, the linopirdine-sensitive outward current activated rapidly and comprised up to 20% of the total current. In current-clamp recordings from GFP+ SO cells, linopirdine induced depolarization and increased AP frequency, whereas retigabine induced hyperpolarization and arrested firing. In multicompartment O-LM interneuron models that incorporated IM, somatodendritic placement of Kv7 channels best reproduced experimentally measured IM. The models suggest that Kv3- and Kv7- mediated channels both rapidly activate during single APs; however, Kv3 channels control rapid repolarization of the AP, whereas Kv7 channels primarily control the interspike interval. [ABSTRACT FROM AUTHOR]

Published

2006